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首页> 外文期刊>Brazilian Journal of Medical and Biological Research >Regulation of protein synthesis and the role of eIF3 in cancer
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Regulation of protein synthesis and the role of eIF3 in cancer

机译:蛋白质合成的调控和eIF3在癌症中的作用

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Maintenance of cell homeostasis and regulation of cell proliferation depend importantly on regulating the process of protein synthesis. Many disease states arise when disregulation of protein synthesis occurs. This review focuses on mechanisms of translational control and how disregulation results in cell malignancy. Most translational controls occur during the initiation phase of protein synthesis, with the initiation factors being the major target of regulation through their phosphorylation. In particular, the recruitment of mRNAs through the m7G-cap structure and the binding of the initiator methionyl-tRNAi are frequent targets. However, translation, especially of specific mRNAs, may also be regulated by sequestration into processing bodies or stress granules, by trans-acting proteins or by microRNAs. When the process of protein synthesis is hyper-activated, weak mRNAs are translated relatively more efficiently, leading to an imbalance of cellular proteins that promotes cell proliferation and malignant transformation. This occurs, for example, when the cap-binding protein, eIF4E, is overexpressed, or when the methionyl-tRNAi-binding factor, eIF2, is too active. In addition, enhanced activity of eIF3 contributes to oncogenesis. The importance of the translation initiation factors as regulators of protein synthesis and cell proliferation makes them potential therapeutic targets for the treatment of cancer.
机译:细胞稳态的维持和细胞增殖的调节主要取决于调节蛋白质合成的过程。当蛋白质合成失调发生时,就会出现许多疾病状态。这篇综述集中在翻译控制的机制以及失调如何导致细胞恶性肿瘤。大多数翻译控制发生在蛋白质合成的起始阶段,起始因子是通过其磷酸化进行调控的主要目标。特别地,通过m7G-cap结构募集mRNA和引发剂甲硫酰基-tRNAi的结合是常见的靶标。但是,也可以通过螯合到加工体或应激颗粒中,通过反式作用蛋白或通过microRNA来调节特别是特定mRNA的翻译。当蛋白质合成过程被高度激活时,较弱的mRNA相对有效地翻译,导致细胞蛋白质失衡,从而促进细胞增殖和恶性转化。例如,当帽结合蛋白eIF4E过表达或甲硫氨酰-tRNAi结合因子eIF2过于活跃时,就会发生这种情况。此外,增强的eIF3活性有助于肿瘤发生。翻译起始因子作为蛋白质合成和细胞增殖的调节剂的重要性使其成为治疗癌症的潜在治疗靶标。

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